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Published:
Journal of Analytical Toxicology,
ISSN 0146-4760,
Volume 31, Number 8, October,
pp.424-433
Prevalence and Disposition of Drugs of
Abuse and Opioid Treatment Drugs in Oral Fluid
Edward J. Cone[1], Joe Clarke [2],
Lolita Tsanaclis[3]
[1]Johns Hopkins School of Medicine, Baltimore, Maryland
[2]Altrix
Healthcare, Ltd., Warrington, United Kingdom
[3]Tricho-Tech, Ltd., Cardiff, United Kingdom
Testing oral fluid for drugs of abuse has been
studied under many conditions but rarely has been evaluated in
large population databases. We evaluated oral fluid tests in
a database from a commercial laboratory in the United Kingdom
composed of 8679 confirmed positive results. The results originated
from 635,000 specimens collected over the period of May 2004
through September 2006. Oral fluid specimens were collected with
the Intercept® oral fluid collection device, screened by
enzyme immunoassay, and confirmed by GC–MS or GC–MS–MS.
The database was organized by collection settings (legal/treatment,
N = 8198 specimens; and workplace, N = 481 specimens) and by
drug groups (without consideration of collection setting). The
drug groups were as follows (number of confirmed positives):
amphetamines (468); benzodiazepines (892); buprenorphine (276);
cannabinoids (725); cocaine (1443); methadone (998); and opiates
(5739). The goal of the study was to provide drug/metabolite
prevalence data, concentrations, and drugs/metabolite patterns
encountered in oral fluid. Comparison of results by collection
setting indicated differences in relative frequency, primarily
for opiates and cannabinoids. Opiate positives were most frequently
observed for specimens collected in legal/treatment settings,
whereas cannabinoids were most frequently reported in the workplace.
An array of information on drug and metabolite occurrences and
concentration arose from evaluation of the data by drug groups.
Amphetamine was the predominant drug reported for the Amphetamines
Group; approximately 10% were also positive for MDA and/or MDMA;
and methamphetamine was rarely reported. Multiple combinations
of diazepam, nordiazepam, oxazepam, temazepam, chlordiazepoxide,
and lorazepam were reported for the Benzodiazepine Group. Buprenorphine,
an opioid treatment drug, was the predominant analyte reported,
but low concentrations of norbuprenorphine were frequently reported.
THC was the predominant analyte reported in the Cannabinoids
Group and was frequently reported in combination with cannabidiol
and cannabinol. THCCOOH was reported in only 10.8% of these specimens
and was never reported in the absence of THC. HO-THC was reported
in 5.7% of the specimens. In the Cocaine Group, cocaine was present,
often in combination with BZE, but also as the sole analyte in
17.3% of the specimens. AEME and cocaethylene were reported in
10.4% and 5.5% of the specimens. Methadone, another opioid treatment
drug, was reported in all specimens for the Methadone Group;
EDDP was reported in 30.1% of the specimens. In the Opiates Group,
morphine, codeine and 6-acetylmorhine were most frequently reported,
often in combination. The frequency of detection of 6-acetylmorphine
when morphine was present (N = 4575 specimens) was 77.5%. Surprisingly,
heroin (19.0%; N = 1091 specimens) and 6-acetylcodeine (24.9%;
N = 1431 specimens) were frequently reported. The results from
analysis of this large oral fluid database offer a rich mixture
of new information on detection frequency, drug and metabolite
patterns, and concentration data on drugs of abuse.
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